| BMC Immunology | |
| The change in Ig regulation from children to adults disconnects the correlation with the 3′RR hs1.2 polymorphism | |
| Domenico Frezza5 Susanna Esposito2 Alessandro Plebani3 Vincenzo Giambra7 Marco Cattalini7 Pietro D’Addabbo1 Renato Massoud4 Andrea Magrini4 Cesare Gargioli5 Valentina Iacoacci5 Laura Porretti2 Nicola Principi2 Cristina Daleno2 Eliseo Serone6 | |
| [1] Department of Biology, University of Bari, Bari, Italy;Department of Pathophysiology and Transplantation, Università degli Studi di Milano, Fondazione IRCCS Ca’ Granda Ospedale Maggiore Policlinico, Milan, Italy;Pediatrics Clinic, Department of Clinical and Experimental Sciences, Università di Brescia e Spedali Civili di Brescia, Brescia, Italy;Department of Sperimental Medicine, Policlinico Tor Vergata, Rome, Italy;Department of Biology “Enrico Calef”, University of Roma Tor Vergata, Rome, 00133, Italy;Department of Life, Health and Environmental Sciences, University of L’Aquila, L’Aquila, Italy;Terry Fox Laboratory, British Columbia Cancer Research Centre, Vancouver, BC, Canada | |
| 关键词: Aging; Transcription factor consensus; SP1; NF-κB; Immune system regulation; Enhancer hs1.2; Immunoglobulin heavy chain; B cell markers; Genotyping; | |
| Others : 1089885 DOI : 10.1186/s12865-014-0045-0 |
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| received in 2014-01-07, accepted in 2014-09-25, 发布年份 2014 | |
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【 摘 要 】
Background
In the immune system, the serum levels of immunoglobulin (Ig) increase gradually during ageing. Through B cell development, the Ig heavy chain expression is modulated by a regulatory region at the 3’ of the constant alpha gene (3’RR), in single copy in rodents and, due to a large duplication, in two copies in apes. The human 3’RR1 and 3’RR2 are both characterized by three enhancers, the central of which, namely hs1.2, is highly polymorphic. Human hs1.2 has four different variants with unique binding sites for transcription factors (e.g. NF-kB and SP1) and shows variable allelic frequencies in populations with immune disorders. In previous works, we have reported that in several autoimmune diseases the *2 allele of hs1.2 is genetically associated to high level of IgM in peripheral blood. In subjects with altered levels of circulating Ig, an increased level was associated to *2 allele of hs1.2 and low levels corresponded to high frequency of *1 allele.
During ageing there is a physiological increase of Ig concentrations in the serum. Therefore, for this study, we hypothesized that the hs1.2 variants may impact differently the levels of secreted Ig during the growth.
Results
We have correlated the allelic frequencies of hs1.2 with IgM, IgG and IgA serum concentrations in two cohorts of healthy people of different age and after three years follow-up in children homozygous for the allele. Here we show that when the expression levels of Ig in children are low and medium, the frequencies of *1 and *2 alleles are the same. Instead, when the Ig expression levels are high, there is a significantly higher frequency of the allele *2. The follow-up of children homozygous for *1 and *2 alleles showed that the increase or decrease of circulating Ig was not dependent on the number of circulating mature B cells.
Conclusions
These data support the idea that under physiologic condition there is a switch of regulative pathways involved in the maturation of Ig during ageing. This mechanism is evidenced by hs1.2 variants that in children but not in adults participate to Ig production, coordinating the three class levels.
【 授权许可】
2014 Serone et al.; licensee BioMed Central Ltd.
【 预 览 】
| Files | Size | Format | View |
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| 20150128152734282.pdf | 336KB |  download |
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| Figure 1. | 47KB | Image | download |
【 图 表 】
Figure 1.
【 参考文献 】
- [1]Orton SM FJ, Bellanti JA: Clinical applications of laboratory diagnostic immunology. In Immunology IV: Clinical Application in Health and Disease. Edited by Bellanti JA. Bethesda MD, I Care Press; 2012.
- [2]Pinaud E, Marquet M, Fiancette R, Peron S, Vincent-Fabert C, Denizot Y, Cogne M: The IgH locus 3′ regulatory region: pulling the strings from behind. Adv Immunol 2011, 110:27-70.
- [3]Giambra V, Volpi S, Emelyanov AV, Pflugh D, Bothwell AL, Norio P, Fan Y, Ju Z, Skoultchi AI, Hardy RR, Frezza D, Birshtein BK: Pax5 and linker histone H1 coordinate DNA methylation and histone modifications in the 3′ regulatory region of the immunoglobulin heavy chain locus. Mol Cell Biol 2008, 28(19):6123-6133.
- [4]Birshtein BK: The role of CTCF binding sites in the 3′ immunoglobulin heavy chain regulatory region. Front Genet 2012, 3:251.
- [5]Rouaud P, Vincent-Fabert C, Saintamand A, Fiancette R, Marquet M, Robert I, Reina-San-Martin B, Pinaud E, Cogne M, Denizot Y: The IgH 3′ regulatory region controls somatic hypermutation in germinal center B cells. J Exp Med 2013, 210(8):1501-1507.
- [6]Chen C, Birshtein BK: Virtually identical enhancers containing a segment of homology to murine 3′IgH-E (hs1,2) lie downstream of human Ig C alpha 1 and C alpha 2 genes. J Immunol 1997, 159(3):1310-1318.
- [7]Chauveau C, Cogne M: Palindromic structure of the IgH 3′locus control region. Nat Genet 1996, 14(1):15-16.
- [8]Saleque S, Singh M, Little RD, Giannini SL, Michaelson JS, Birshtein BK: Dyad symmetry within the mouse 3′ IgH regulatory region includes two virtually identical enhancers (C alpha3′E and hs3). J Immunol 1997, 158(10):4780-4787.
- [9]D'Addabbo P, Scascitelli M, Giambra V, Rocchi M, Frezza D: Position and sequence conservation in Amniota of polymorphic enhancer HS1.2 within the palindrome of IgH 3′Regulatory Region. BMC Evol Biol 2011, 11:71. BioMed Central Full Text
- [10]Mills FC, Harindranath N, Mitchell M, Max EE: Enhancer complexes located downstream of both human immunoglobulin Calpha genes. J Exp Med 1997, 186(6):845-858.
- [11]Giambra V, Fruscalzo A, Giufre M, Martinez-Labarga C, Favaro M, Rocchi M, Frezza D: Evolution of human IgH3′EC duplicated structures: both enhancers HS1,2 are polymorphic with variation of transcription factor's consensus sites. Gene 2005, 346:105-114.
- [12]Frezza D, Tolusso B, Giambra V, Gremese E, Marchini M, Nowik M, Serone E, D'Addabbo P, Mattioli C, Canestri S, Petricca L, D’Antona G, Birshtein BK, Scorza R, Ferraccioli G: Polymorphisms of the IgH enhancer HS1.2 and risk of systemic lupus erythematosus. Ann Rheum Dis 2012, 71(8):1309-1315.
- [13]Frezza D, Giambra V, Cianci R, Fruscalzo A, Giufre M, Cammarota G, Martinez-Labarga C, Rickards O, Scibilia G, Sferlazzas C, Bartolozzi F, Starnino S, Magazzu G, Gasbarrini GB, Pandolfi F: Increased frequency of the immunoglobulin enhancer HS1,2 allele 2 in coeliac disease. Scand J Gastroenterol 2004, 39(11):1083-1087.
- [14]Cianci R, Giambra V, Mattioli C, Esposito M, Cammarota G, Scibilia G, Magazzu G, Orlando A, Sandri G, Bianchi L, Gasbarrini GB, Pandolfi F, Frezza D: Increased frequency of Ig heavy-chain HS1,2-A enhancer *2 allele in dermatitis herpetiformis, plaque psoriasis, and psoriatic arthritis. J Invest Dermatol 2008, 128(8):1920-1924.
- [15]Tolusso B, Frezza D, Mattioli C, Fedele AL, Bosello S, Faustini F, Peluso G, Giambra V, Pietrapertosa D, Morelli A, Gremese E, De Santis M, Ferraccioli GF: Allele *2 of the HS1,2A enhancer of the Ig regulatory region associates with rheumatoid arthritis. Ann Rheum Dis 2009, 68(3):416-419.
- [16]Giambra V, Cianci R, Lolli S, Mattioli C, Tampella G, Cattalini M, Kilic SS, Pandolfi F, Plebani A, Frezza D: Allele *1 of HS1.2 enhancer associates with selective IgA deficiency and IgM concentration. J Immunol 2009, 183(12):8280-8285.
- [17]Fernando TM, Ochs SD, Liu J, Chambers-Turner RC, Sulentic CE: 2,3,7,8-tetrachlorodibenzo-p-dioxin induces transcriptional activity of the human polymorphic hs1,2 enhancer of the 3′Igh regulatory region. J Immunol 2012, 188(7):3294-3306.
- [18]Giambra V, Martinez-Labarga C, Giufre M, Modiano D, Simpore J, Gisladottir BK, Francavilla R, Zhelezova G, Kilic SS, Crawford M, Biondi G, Rickards O, Frezza D: Immunoglobulin enhancer HS1,2 polymorphism: a new powerful anthropogenetic marker. Ann Hum Genet 2006, 70(Pt 6):946-950.
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